家族性单纯性近端肾小管酸中毒——一项临床与遗传学研究。

Familial pure proximal renal tubular acidosis--a clinical and genetic study.

作者信息

Katzir Ze'ev, Dinour Dganit, Reznik-Wolf Haike, Nissenkorn Andrea, Holtzman Eliezer

机构信息

Ze'ev Katzir, Pediatric Nephrology Services, E. Wolfson Medical Center, Holon, Israel.

出版信息

Nephrol Dial Transplant. 2008 Apr;23(4):1211-5. doi: 10.1093/ndt/gfm583. Epub 2007 Sep 19.

DOI:10.1093/ndt/gfm583

PMID:17881426

Abstract

BACKGROUND

Inherited proximal renal tubular acidosis (pRTA) is commonly associated with more generalized proximal tubular dysfunctions and occasionally with other organ system defects. Inherited combined pRTA and distal RTA with osteopetrosis and pure pRTA associated with ocular abnormalities, a rare disease which has been recently described. Only one family with pure isolated pRTA has been reported so far and the genetic cause for this disease is unknown. Objectives. We report a unique family with isolated pRTA. The aim of the project was to define the phenotype and to try to find the gene defect causing the disease.

METHODS

Clinical and metabolic evaluation of all family members was performed and a family pedigree was constructed. DNA was extracted from blood samples of affected and unaffected family members. We amplified by PCR and sequenced the coding areas and splice-sites of the genes that contribute to HCO(-)(3) reclamation in the proximal tubule. The genes studied were as follows: CA II, CA IV, CA XIV, NCB1, Na(+)/H(+) exchanger (NHE)-3, NHE-8, the regulatory proteins of NHE3, NHRF1 and NHRF2 and the Cl(-)/HCO(-)(3) exchanger, SLC26A6.

RESULTS

The father and all four children had RTA with blood HCO(-)(3) levels of 11-14 meq/l and urine pH of 5.3-5.4. Increased HCO(-)(3) fractional excretion after bicarbonate loading to 40-60% confirmed the diagnosis pRTA. No other tubular dysfunction was found, and no organ system dysfunction was detected, besides short stature. No mutation was found in all candidate genes studied.

CONCLUSIONS

We presented a second family in the literature with familial isolated pure pRTA. The mode of inheritance is compatible with an autosomal dominant disease. Because of the small size of the family, wide genome search was not applicable and the gene candidate approach was chosen. Nine important candidate genes were extensively studied but the molecular basis of the disease was not yet found and genotyping nine important gene candidates were negative.

摘要

背景

遗传性近端肾小管酸中毒（pRTA）通常与更广泛的近端肾小管功能障碍相关，偶尔也与其他器官系统缺陷有关。遗传性联合pRTA和远端RTA伴骨硬化以及与眼部异常相关的纯pRTA，是一种最近才被描述的罕见疾病。迄今为止，仅报道过一个患有纯孤立性pRTA的家族，且该疾病的遗传原因尚不清楚。目的。我们报告一个患有孤立性pRTA的独特家族。该项目的目的是确定其表型，并试图找到导致该疾病的基因缺陷。

方法

对所有家庭成员进行临床和代谢评估，并构建家系图谱。从患病和未患病家庭成员的血液样本中提取DNA。我们通过PCR扩增并对参与近端小管中HCO(-)(3)重吸收的基因的编码区和剪接位点进行测序。所研究的基因如下：碳酸酐酶II（CA II）、碳酸酐酶IV（CA IV）、碳酸酐酶XIV（CA XIV）、NBC1、钠/氢交换体（NHE）-3、NHE-8、NHE3的调节蛋白、NHRF1和NHRF2以及氯/碳酸氢根交换体（Cl(-)/HCO(-)(3) exchanger）、SLC26A6。

结果

父亲和所有四个孩子均患有RTA，血液HCO(-)(3)水平为11 - 14 meq/l，尿液pH值为5.3 - 5.4。给予碳酸氢盐负荷后HCO(-)(3)分数排泄增加至40 - 60%，证实了pRTA的诊断。除身材矮小外，未发现其他肾小管功能障碍，也未检测到器官系统功能障碍。在所研究的所有候选基因中均未发现突变。